Hypothesis:
Pharmacologic inhibition of AR-V7 will be a valuable therapeutic strategy for patients with mCRPC. Our overall aim is to investigate the mechanism of action and determine the therapeutic potential of selective AR-V7 inhibitors in vitro and in vivo.
Specific Aims:
Perform medicinal chemistry for lead compound optimization and determine compound mechanism of action.
Investigate compound in vivo activity in CRPC xenografts and established models of enzalutamide-resistance.
Specific Aims:
Hypothesis:
Beyond promoting established PCa growth and metastasis, dysregulated UBR5 expression may play a strong role in the transformation and malignant development of the normal prostate.
Specific Aim:
To develop a novel genetically engineered mouse model (GEMM) of UBR5-driven prostate cancer. This model will be based the loss of function of the tumor suppressor Pten together with a gain of UBR5 expression.
Hypothesis:
The application of avail able statistical methods, in combination with prostate cancer PRS derivation in a population with ade quate minority population sample size, will mitigate the significant prostate-cancer PRS population port ability problems and generate a prostate cancer PRS applicable to a Black-race population.
Specific Aims:
Assessment of multi-ethnic prostate cancer PRSs
Systematic Comparison of Correction Methods
Inquiry of Population-Specific Mitigation Strategies
